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首页> 外文期刊>Inhalation toxicology >Differences in the toxicity of cerium dioxide nanomaterials after inhalation can be explained by lung deposition, animal species and nanoforms
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Differences in the toxicity of cerium dioxide nanomaterials after inhalation can be explained by lung deposition, animal species and nanoforms

机译:吸入后二氧化铈纳米材料的毒性的差异可以通过肺沉积,动物物种和纳米血管来解释

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Considerable differences in pulmonary responses have been observed in animals exposed to cerium dioxide nanoparticles via inhalation. These differences in pulmonary toxicity might be explained by differences in lung deposition, species susceptibility or physicochemical characteristics of the tested cerium dioxide nanoforms (i.e. same chemical substance, different size, shape, surface area or surface chemistry). In order to distinguish the relative importance of these different influencing factors, we performed a detailed analysis of the data from several inhalation studies with different exposure durations, species and nanoforms, namely published data on NM211 and NM212 (JRC repository), NanoAmor (commercially available) and our published and unpublished data on PROM (industry provided). Data were analyzed by comparing the observed pulmonary responses at similar external and internal dose levels. Our analyses confirm that rats are more sensitive to developing pulmonary inflammation compared to mice. The observed differences in responses do not result purely from differences in the delivered and retained doses (expressed in particle mass as well as surface area). In addition, the different nanoforms assessed showed differences in toxic potency likely due to differences in their physicochemical parameters. Primary particle and aggregate/agglomerate size distributions have a substantial impact on the deposited dose and consequently on the pulmonary response. However, in our evaluation size could not fully explain the difference observed in the analyzed studies indicating that the pulmonary response also depends on other physicochemical characteristics of the particles. It remains to be determined to what extent these findings can be generalized to other poorly soluble nanomaterials.
机译:通过吸入地暴露于二氧化铈纳米颗粒的动物中观察到肺反应的相当大的差异。这些肺毒性的差异可以通过肺部沉积,物种敏感性或测试二氧化铈纳米摩的物种(即相同的化学物质,不同尺寸,形状,表面积或表面化学)来解释。为了区分这些不同影响因素的相对重要性,我们对来自不同曝光持续性,物种和纳米型的几种吸入研究进行了详细分析,即在NM211和NM212(JRC储存库),纳米摩尔(可商购) )以及我们关于PROM(提供的行业)的发布和未发表的数据。通过比较在类似的外部和内剂量水平下观察到的肺反应进行分析数据。我们的分析证实,与小鼠相比,大鼠对发育肺炎症更敏感。观察到的反应差异不会纯粹从递送和保留剂量的差异(以颗粒物质和表面积表示)。此外,评估的不同纳米型显示出由于其物理化学参数的差异而言,可能的毒性效力可能存在差异。初级颗粒和骨料/聚集尺寸分布对沉积剂量具有显着影响,因此对肺反应产生了显着影响。然而,在我们的评估规模中,不能完全解释分析的研究中观察到的差异,表明肺反应也取决于颗粒的其他物理化学特征。仍有待确定这些发现可以在多大程度上推广到其他不良型纳米材料中。

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